A discussion about the limitations of the Eurocode’s high-speed load model for railway bridges

High-speed railway bridges are subjected to normative limitations concerning maximum permissible deck accelerations.For the design of these structures,the European norm EN 1991-2 introduces the high-speed load model(HSLM)—a set of point loads intended to include the effects of existing high-speed trains.Yet,the evolution of current trains and the recent development of new load models motivate a discussion regarding the limits of validity of the HSLM.For this study,a large number of randomly generated load models of articulated,conventional,and regular trains are tested and compared with the envelope of HSLM effects.For each type of train,two sets of 100,000 load models are considered:one abiding by the limits of the EN 1991-2 and another considering wider limits.This comparison is achieved using both a bridge-independent metric(train signatures)and dynamic analyses on a case study bridge(the Canelas bridge of the Portuguese Railway Network).For the latter,a methodology to decrease the computational cost of moving loads analysis is introduced.Results show that some theoretical load models constructed within the stipulated limits of the norm can lead to effects not covered by the HSLM.This is especially noted in conventional trains,where there is a relation with larger distances between centres of adjacent vehicle bogies.

Rifaximin on epigenetics and autophagy in animal model of hepatocellular carcinoma secondary to metabolic-dysfunction associated steatotic liver disease

BACKGROUND Prevalence of hepatocellular carcinoma(HCC)is increasing,especially in patients with metabolic dysfunctionassociated steatotic liver disease(MASLD).AIM To investigate rifaximin(RIF)effects on epigenetic/autophagy markers in animals.METHODS Adult Sprague-Dawley rats were randomly assigned(n=8,each)and treated from 5-16 wk:Control[standard diet,water plus gavage with vehicle(Veh)],HCC[high-fat choline deficient diet(HFCD),diethylnitrosamine(DEN)in drinking water and Veh gavage],and RIF[HFCD,DEN and RIF(50 mg/kg/d)gavage].Gene expression of epigenetic/autophagy markers and circulating miRNAs were obtained.RESULTS All HCC and RIF animals developed metabolic-dysfunction associated steatohepatitis fibrosis,and cirrhosis,but three RIF-group did not develop HCC.Comparing animals who developed HCC with those who did not,miR-122,miR-34a,tubulin alpha-1c(Tuba-1c),metalloproteinases-2(Mmp2),and metalloproteinases-9(Mmp9)were significantly higher in the HCC-group.The opposite occurred with Becn1,coactivator associated arginine methyltransferase-1(Carm1),enhancer of zeste homolog-2(Ezh2),autophagy-related factor LC3A/B(Map1 Lc3b),and p62/sequestosome-1(p62/SQSTM1)-protein.Comparing with controls,Map1 Lc3b,Becn1 and Ezh2 were lower in HCC and RIF-groups(P<0.05).Carm1 was lower in HCC compared to RIF(P<0.05).Hepatic expression of Mmp9 was higher in HCC in relation to the control;the opposite was observed for p62/Sqstm1(P<0.05).Expression of p62/SQSTM1 protein was lower in the RIF-group compared to the control(P=0.024).There was no difference among groups for Tuba-1c,Aldolase-B,alpha-fetoprotein,and Mmp2(P>0.05).miR-122 was higher in HCC,and miR-34a in RIF compared to controls(P<0.05).miR-26b was lower in HCC compared to RIF,and the inverse was observed for miR-224(P<0.05).There was no difference among groups regarding miR-33a,miR-143,miR-155,miR-375 and miR-21(P>0.05).CONCLUSION RIF might have a possible beneficial effect on preventing/delaying liver carcinogenesis through epigenetic modulation in a rat model of MASLD-HCC.

Ornithine aspartate effects on bacterial composition and metabolic pathways in a rat model of steatotic liver disease

BACKGROUND Metabolic-dysfunction associated steatotic liver disease(MASLD)is a hepatic manifestation of metabolic syndrome.Studies suggest ornithine aspartate(LOLA)as drug therapy.AIM To analyze the influence of LOLA intake on gut microbiota using a nutritional model of MASLD.METHODS Adult male Sprague Dawley rats were randomized into three groups:Control(10 rats fed with a standard diet),MASLD(10 rats fed with a high-fat and choline-deficient diet),and LOLA(10 rats receiving 200 mg/kg/d LOLA,after the 16th week receiving high-fat and choline-deficient diet).After 28 wk of the experiment,animals were euthanized,and feces present in the intestine were collected.Following fecal DNA extraction,the V4 region of the 16S rRNA gene was amplified followed by sequencing in an Ion S5™system.RESULTS Alpha and beta diversity metrics were comparable between MASLD and LOLA.3 OTUs were differentially abundant between MASLD and LOLA,which belong to the species Helicobacter rodentium,Parabacteroides goldsteinii,and Parabacteroides distasonis.The functional prediction provided two different metabolic profiles between MASLD and LOLA.The 9 pathways differentially abundant in MASLD are related to a change in energy source,adenosine/purine nucleotides degradation as well as guanosine and adenosine deoxyribonucleotides biosynthesis.The 14 pathways differentially abundant in LOLA are associated with four major metabolic functions primarily influenced by L-aspartate,including tricarboxylic acid cycle pathways,purine/guanosine nucleotides biosynthesis,pyrimidine ribonucleotides biosynthesis and salvage as well as lipid IVA biosynthesis.CONCLUSION Although LOLA had no influence on alpha and beta diversity in this nutritional model of MASLD,it was associated with changes in specific gut microbes and their related metabolic pathways.

FibroScan-aspartate transaminase:A superior non-invasive model for diagnosing high-risk metabolic dysfunction-associated steatohepatitis

BACKGROUND Non-alcoholic fatty liver disease(NAFLD)with hepatic histological NAFLD activity score≥4 and fibrosis stage F≥2 is regarded as“at risk”non-alcoholic steatohepatitis(NASH).Based on an international consensus,NAFLD and NASH were renamed as metabolic dysfunction-associated steatotic liver disease(MASLD)and metabolic dysfunction-associated steatohepatitis(MASH),respectively;hence,we introduced the term“high-risk MASH”.Diagnostic values of seven non-invasive models,including FibroScan-aspartate transaminase(FAST),fibrosis-4(FIB-4),aspartate transaminase to platelet ratio index(APRI),etc.for high-risk MASH have rarely been studied and compared in MASLD.AIM To assess the clinical value of seven non-invasive models as alternatives to liver biopsy for diagnosing high-risk MASH.METHODS A retrospective analysis was conducted on 309 patients diagnosed with NAFLD via liver biopsy at Beijing Ditan Hospital,between January 2012 and December 2020.After screening for MASLD and the exclusion criteria,279 patients wereincluded and categorized into high-risk and non-high-risk MASH groups.Utilizing threshold values of each model,sensitivity,specificity,positive predictive value(PPV),and negative predictive values(NPV),were calculated.Receiver operating characteristic curves were constructed to evaluate their diagnostic efficacy based on the area under the curve(AUROC).RESULTS MASLD diagnostic criteria were met by 99.4%patients with NAFLD.The MASLD population was analyzed in two cohorts:Overall population(279 patients)and the subgroup(117 patients)who underwent liver transient elastography(FibroScan).In the overall population,FIB-4 showed better diagnostic efficacy and higher PPV,with sensitivity,specificity,PPV,NPV,and AUROC of 26.9%,95.2%,73.5%,72.2%,and 0.75.APRI,Forns index,and aspartate transaminase to alanine transaminase ratio(ARR)showed moderate diagnostic efficacy,whereas S index and gamma-glutamyl transpeptidase to platelet ratio(GPR)were relatively weaker.In the subgroup,FAST had the highest diagnostic efficacy,its sensitivity,specificity,PPV,NPV,and AUROC were 44.2%,92.3%,82.1%,67.4%,and 0.82.The FIB-4 AUROC was 0.76.S index and GPR exhibited almost no diagnostic value for high-risk MASH.CONCLUSION FAST and FIB-4 could replace liver biopsy as more effectively diagnostic methods for high-risk MASH compared to APRI,Forns index,ARR,S index,and GPR;FAST is superior to FIB-4.

Analysis of the Application Effect of Family Collaborative Care Model on Elderly Patients with Type 2 Diabetes Mellitus and the Situation of Self-Care Ability

Objective: To study the application effect of the family collaborative care model on elderly patients with type 2 diabetes mellitus and its influence on self-care ability. Methods: The elderly type 2 diabetes mellitus patients (400 cases) treated in our hospital between March 2020 and July 2023 were divided into two groups by randomized grouping method;the control group received the conventional nursing program, while the observation group received the family collaborative nursing model. Blood glucose level, self-care ability, and quality of life were compared between the groups. Results: The blood glucose level of the observation group was lower than that of the control group (P < 0.05). The self- care ability and quality of life scores of the observation group were higher than those of the control group (P < 0.05). Conclusion: The family collaborative care model for elderly patients with type 2 diabetes mellitus can promote their self- care ability, improve the effect of glycemic control, and improve their quality of life, and is suitable for further promotion and application.

新生儿ABO*A2.08亚型等位基因的鉴定及蛋白结构分析

目的:研究ABO*A2.08亚型的血清学特征和蛋白结构,探究其遗传学分子机制。方法:利用血清学方法对先证者及其家系成员进行ABO血型鉴定,应用聚合酶链反应-序列特异性方法进行ABO基因分型,并对ABO基因第6、7外显子直接测序分析,通过同源蛋白保守性分析、3D分子建模和蛋白稳定性预测探究A2.08亚型中基因突变对GTA蛋白结构稳定性的影响。结果:先证者血清学结果为Ax亚型,ABO基因分型明确先证者的基因型为ABO*A207/08;先证者的父亲基因测序结果证实ABO基因第7外显子存在c.539G>C特征性变异,导致多肽链p.Arg180Pro(R180P)替换。3D蛋白分子建模与分析提示R180P突变后蛋白结构中局部氨基酸的氢键数目发生改变,蛋白稳定性预测显示该突变对蛋白结构稳定性影响较大。结论:ABO基因第7外显子c.539G>C突变导致多肽链氨基酸替换,影响了GTA蛋白结构的稳定性,引起酶活性改变,产生A2.08表型,且该变异基因可稳定遗传。

表观遗传修饰对ABO基因表达影响的研究进展

ABO血型的精准鉴定对临床安全输血至关重要。血清学和基因分型技术的应用使疑难血型鉴定问题得到一定程度的解决,但临床仍有表型与基因型不匹配的问题存在,影响血型鉴定和有效输血。表观遗传修饰是调控基因表达的重要方式,包括DNA甲基化、组蛋白修饰和非编码RNA调控。ABO基因的表达受到表观遗传机制的调控,因此表观遗传修饰对ABO基因表达的影响可能是这部分血型难以鉴定的分子机制之一。DNA甲基化水平对ABO基因表达影响的研究较多,但有关其他表观遗传修饰机制的研究较少,尤其是多种类型的非编码RNA被发现,它们对ABO基因表达的调控机制需要更多的研究进行探讨。

质量监测指标在血站实验室ABO血型检测中的应用

目的分析ABO血型检测相关质量监测指标情况及其变化趋势,探讨质量监测指标在血站实验室ABO血型检测过程中的作用。方法以该中心2012—2021年2733642例献血者标本为研究对象,分析2012—2021年ABO血型检测过程中相关质量监测指标,包括特殊血型检出率、标本血型与血液制剂血型不一致率、采血部门血型检测错误率、送检血型与确认结果符合率等,对数据进行整理和分析。结果2012—2021年2733642例献血者特殊血型检出率中位数为0.030%,各年度比较,差异有统计学意义(0.019%~0.051%;χ^(2)=75.612,P<0.01)。标本血型与血液制剂血型不一致率为0.04■,各年度比较,差异有统计学意义(0.00■~0.21■;χ^(2)=15.787,P<0.01),呈递减趋势(χ^(2)=11.178,P<0.01)。采血部门血型检测错误率为0.55?,各年度比较,差异有统计学意义(0.24■~0.77■;χ^(2)=18.247,P<0.05),呈递减趋势(χ^(2)=8.143,P<0.01)。送检血型与确认结果符合率为78.24%,各年度比较,差异无统计学意义(70.94%~84.71%,χ^(2)=11.993,P>0.05),未见明显趋势变化(χ^(2)=0.879,P>0.05)。结论血站实验室应使用质量监测指标对ABO血型检测进行持续监控和过程评价,确保实验室检测能力的有效性、稳定性,为血型检测过程管理持续改进提供数据依据。

33例非O型ABOi肾移植受者围术期血型抗体的变化

目的统计分析非O型ABO血型不相合肾移植(ABOi-KT)受者围手术期结果资料,旨在探寻ABOi-KT患者血浆中血型抗体的变化情况。方法回顾性分析本院2021年1月—2023年10月首次肾移植、血型仅为A型和B型的33对ABOi-KT供、受体的临床资料,供者血型均为AB型,依据受者血型的不同,分为AB供A组(n=18)和AB供B组(n=15)。分析比较术前血浆置换对2组患者抗体效价的影响,术后2组患者血型抗体反弹和肾功能指标(术后d 1、3、7、14的尿素氮、肌酐和肾小球滤过率)的差异。依据术后血型抗体反弹与否,分为抗体反弹组(n=7)和非反弹组(n=26),分析比较初始效价在血型抗体反弹和非反弹组的差异。结果术前血浆置换对患者IgM抗体的清除率在2组间的差异无统计学意义(Z=-0.260,P>0.05);术后d 1、3、7、14,2组患者肾功指标均无统计学差异;AB供B组术后更易出现血型抗体效价反弹(P<0.05);初始IgM抗体效价在血型抗体反弹组和非反弹组有统计学差异(Z=-2.127,P<0.05),但是初始IgG抗体效价(Z=-1.835,P>0.05)在2组间无统计学意义。结论与AB供A组相比,术后AB供B的患者更易发生血型抗体效价反弹。

ABO血型变异的分子基础研究

目的 对临床ABO血型变异标本进行ABO亚型、类孟买血型与基因型关联性研究,以探讨这2种血型产生的可能分子背景,为ABO血型的准确鉴定与预判提供精确的基因检测靶点和理论依据。方法 对2022年2—12月瑞金医院2.42万名血型鉴定患者,以及期间来自外院送检10例ABO疑难标本(疑似ABO亚型3例,疑似类孟买血型7例)进行血清学分析,对血清学鉴定为ABO亚型、类孟买血型的行DNA直接测序或克隆后测序分析ABO、FUT1、FUT2基因序列。结果 在共计2.42万血型鉴定患者中检出7例ABO亚型;外院送检的10例疑难标本检出2例ABO亚型、1例正常A型、7例类孟买血型。我们共鉴定出:1)9例ABO亚型,表型及其对应基因型分别为:1例A_(el)(AEL.02/O.01.02)、1例A_(el)B(AEL.05/B.01)、3例B_(3)(2例B3.03/O.01.01、1例B3.03/O.01.02)、1例B(A)(BA.02/O.01.01)、1例AB_(weak)(A1.02/BW.07)、1例B_(weak)(BW.31/O.01.02)、1例A_(2)B_(weak)(A2.05/BW.31);2)7例类孟买血型,表型及其对应基因型分别为:1例AB_(m)^(h)(FUT1^(*)01N.13/FUT1^(*)01N.13)、4例A_(m)^(h)(3例FUT1^(*)01N.06/FUT1^(*)01N.13、1例FUT1^(*)01N.13/FUT1^(*)01N.13)、2例B_(m)^(h)(FUT1^(*)01N.06/FUT1^(*)01N.06、FUT1^(*)01N.06/FUT1^(*)01N.13),7例类孟买的FUT2基因型均为FUT2^(*)01/FUT2^(*)01。结论 ABO血型变异标本需联合血清学与分子生物学方法进行鉴定,方能提高对血型变异标本的鉴定准确率,从而为临床安全输血、器官移植、胎母免疫性溶血病的预测与防治提供参考。

2021—2022年广州地区献血人群ABO血型筛查结果分析

目的 了解广州地区无偿献血者ABO、RhD血型的分布情况,为保证临床用血安全和更好为献血者服务提供依据。方法 对2021年1月—2022年12月的无偿献血者进行常规ABO、RhD血型检测,统计分析ABO血型构成比,对ABO正反不一致血型、RhD初筛阴性的标本进行血型血清学确证,分析ABO亚型检出情况及漏检原因。结果 2021年1月—2022年12月共筛查献血者标本749 123份,剔除重复献血者后的标本513 291份,其中ABO血型分布为:O型208 126份(40.55%)、A型138 859份(27.05%)、B型130 987份(25.52%)、AB型35 319份(6.88%)。ABO血型初筛正反不一致506份,其中弱/无红细胞反应58份、额外的红细胞反应16份、弱/无血清反应215份、额外的血清反应217份;经血型血清学或分子生物学确认ABO亚型44份,其中A亚型13份、B亚型26份、AB亚型5份;B(A)3份;类孟买血型14份。重复献血者漏检率最高的血型是A_3/B_3类亚型(68.42%)。在513 291份标本中共检出意外抗体阳性128份;RhD血型初筛阴性共2 277份,其中RhD阴性确认2 188份[2 188/513 291(0.43%)],RhD变异型89份[89/513 291(0.02%)],合并检出意外抗体30份[30/2 188(1.37%)]。结论 广州地区献血人群ABO分布O>A>B>AB,RhD阴性人群占比为0.43%,略高于全国汉族人群0.3%~0.4%;ABO血型亚型以B亚型为主;A_3/B_3类亚型的检出率及在常规血型检验中漏检率最高。

血清学检测和基因分型在ABO疑难血型鉴定中的性能评价

目的分析血清学检测和基因分型在ABO疑难血型鉴定中的应用。方法对106例ABO疑难血型实施血清学检测(吸收放散试验)等,同时对其实施基因分型检测(荧光定量PCR试验),以基因测序结果为金标准,评估血清学检测和基因分型所得结果与基因测序一致性,比较两种检查方式灵敏度、特异度。结果以基因测序为金标准,血清学检测所得结果一致性为中度,基因分型检测所得结果一致性很好。通过比较血清学检测和基因分型灵敏度、特异度可知,两种检查方式所得特异度、灵敏度差异有统计学意义,基因分型灵敏度、特异度更高(P<0.05)。结论基因分型检测和血清学检测有各自的优缺点,但总体上来说,基因分型检测具有更高的准确性和可靠性,更快速、高效。

ABO基因第7外显子c.539G>C突变致A_(2)B亚型结果分析

目的:探讨ABO基因第7外显子c.539G>C突变致A_(2)B亚型结果分析。方法:采用试管凝集法检测ABO血型,采用Sanger测序法进行基因测序及序列分析。结果:4例先证者红细胞为A弱B表型,根据血清学特征定义为A_(2)B血型,先证者1、3、4血清中无抗-A_(1)抗体;先证者2血清中存在抗-A_(1)抗体;4例血型基因型为ABO^(*)A2.08/ABO^(*)B.01,测序结果与A102基因序列比对,A208在c.467C>T和c.539G>C位发生突变,导致多肽链P156L和R180P替换。结论:α-1,3-N-乙酰半乳糖胺转移酶基因c.539G>C突变产生A208表型。

影响ABO血型鉴定的红细胞同种抗体的种类分布与分析

目的探讨不同血型系统同种抗体对ABO血型鉴定的影响。方法选取2014年1月至2021年12月中国医学科学院肿瘤医院ABO血型正反定型不符且通过实验确定为由同种抗体干扰所致的患者标本。选择抗体对应抗原阴性的红细胞进行ABO血型鉴定,准确确定患者血型。结果209例同种抗体干扰ABO血型的患者中,卡式抗体筛查阳性146例(69.9%),阴性63例(30.1%);其中抗-M(85例,40.7%)最多,其次为抗-P1(61例,29.2%)、Lewis系统抗体(39例,18.7%)和Rh系统抗体(20例,9.6%)。选择抗体对应抗原阴性的红细胞进行ABO血型鉴定可有效排除同种抗体对血型鉴定的干扰。结论干扰血型鉴定的同种抗体以IgM类盐水抗体为主,主要包括抗-M、抗-P1和Lewis系统抗体,少量IgG类抗体也会干扰血型鉴定,主要是Rh系统抗体。

采用STAMP-24Model的多组织事故分析

安全生产事故往往由多组织交互、多因素耦合造成,事故原因涉及多个组织。为预防和遏制多组织生产安全事故的发生,基于系统理论事故建模与过程模型(Systems-Theory Accident Modeling and Process,STAMP)、24Model,构建一种用于多组织事故分析的方法,并以青岛石油爆炸事故为例进行事故原因分析。结果显示:STAMP-24Model可以分组织,分层次且有效、全面、详细地分析涉及多个组织的事故原因,探究多组织之间的交互关系;对事故进行动态演化分析,可得到各组织不安全动作耦合关系与形成的事故失效链及管控失效路径,进而为预防多组织事故提供思路和参考。

基于改进24Model-ISM-SNA建筑工人不安全行为关联路径研究

建筑施工现场环境复杂,为有效控制不安全行为发生,基于行为安全“2-4”模型对360份具有代表性的建筑安全事故调查报告进行分析,提取出22个不安全行为的主要影响因素。利用灰色关联分析方法(GRA)改进的集成ISM-SNA模型,将不安全行为风险因素划分为表层、过渡层与深层,然后对风险因素进行可视化分析、中心度分析及凝聚子群分析,揭示了各致因因素间的关联关系和传导路径。结果表明,建筑工人不安全行为影响因素可划分成7级3阶的多级递阶结构,安全意识、现场监管、外部环境是建筑工人不安全行为的关键影响因素,同时现场监管和隐患排查到位能有效降低不安全行为的发生。

基于24Model-D-ISM的地铁站火灾疏散影响因素研究

为预防地铁站火灾事故,深入了解地铁站火灾人员疏散影响因素间的内在联系与层次结构,基于第6版“2-4”模型(24Model)分析63起地铁站火灾疏散事故,充分考虑各个因素之间的交互作用,提取19个影响地铁站人员疏散的关键因素,建立地铁站火灾人员疏散影响因素指标体系;采用算子客观赋权法(C-OWA)改进决策试验与评价实验法(DEMATEL),确定地铁站火灾人员疏散的重要影响因素;在此基础上,采用解释结构模型(ISM)分析各个因素间的层次结构及相互作用路径,构建地铁站火灾人员疏散影响因素的多级递阶结构模型。研究结果表明:疏散引导、恐慌从众行为、人员拥挤为地铁站火灾人员疏散的关键影响因素;地铁站火灾人员疏散受表层因素、中间层因素、深层因素共同作用的影响,其中,疏散教育与培训、设施维护与检查、疏散预案等因素是根源影响因素,重视根源影响因素的改善有利于从本质上预防和控制事故的发生。

微柱凝胶技术与凝聚胺技术在ABO新生儿溶血病输血前检测中应用对比

目的对比分析微柱凝胶技术与凝聚胺技术在ABO新生儿溶血病输血前检测中的应用。方法将郑州市第一人民医院2020年1月至2023年5月ABO新生儿溶血病患儿(88例)作为研究对象,依据区间随机法将其分为对照组、研究组,各纳入44例,对照组行输血治疗前开展凝聚胺技术检验血型配血,研究组输血治疗前开展微柱凝胶技术检验血型配血。比较两组检验符合率、一次性交叉配血成功率。结果研究组正定型、反定型符合率(100.00%、100.00%)均高于对照组(86.36%、86.36%),两组差异有统计学意义(P<0.05);研究组交叉配血成功率(100.00%)高于对照组(86.36%),两组差异有统计学意义(P<0.05)。结论对比凝聚胺技术,微柱凝胶技术在ABO新生儿溶血病输血前检测中的应用价值更高,有利于提升输血安全,值得应用。

ABO血型基因外显子1上新变异的鉴定

目的:应用血清学和分子生物学方法鉴定1例ABO正反定型不一致患者的血型,并探讨其遗传学特点。方法:采用试管法鉴定该患者的ABO表型,荧光PCR法测定患者及其父母的ABO血型基因型,并对ABO基因7个外显子进行直接测序分析。结果:本例患者血清学初步鉴定为Bel亚型;基因分型检测患者及其父亲的基因型为B/O1,其母亲的基因型为O1/O1;测序发现在患者及其父亲ABO基因外显子1上有新的c.16_17delins TGTTGCA杂合变异。结论:外显子1上新的变异导致该患者ABO血型出现Bel亚型,并具有遗传性。

ABO次侧不相合血小板输注的有效性和安全性初步研究

目的研究分析紧急特殊情况下ABO次侧不相合血小板输注的有效性与安全性,为ABO次侧不相合血小板输注提供科学依据。方法①收集2013年1月—2023年6月广州市第一人民医院,深圳市中西医结合医院及广东医科大学附属第二医院紧急特殊情况下的24人次ABO次侧不相合血小板输注,为ABO次侧不相合组;收集同期ABO同型血小板输注610人次,用倾向评分匹配的方法从中筛选出拥有相似特征的24人次ABO同型血小板输注,为ABO同型组。比较两组间血小板输注疗效,患者住院天数及肝肾功能等指标的差异,分析ABO次侧不相合组急性溶血性输血反应发生率。②体外模拟受血者输注ABO次侧不相合血小板,盐水介质法检测输注后的红细胞凝集强度。结果①回顾分析中ABO次侧不相合组的血小板差值(ΔPLT)和血小板回收率(PPR)分别为(18.0±20.2)×10^(9)/L,(55.4±54.5)%;ABO同型组则分别为(20.6±15.4)×10^(9)/L,(61.9±48.9)%,以上指标两组间无统计学差异,t值分别为0.51,0.46,P均>0.05。②ABO次侧不相合组患者的住院天数,谷丙转氨酶(ALT),肌酐(Cr),IgG免疫球蛋白,IgM免疫球蛋白,CD4计数,CD8计数及B淋巴细胞计数分别为(30.4±17.8)d,(33.0±16.3)U/L,(104.9±64.7)μmol/L,(9.1±2.6)g/L,(1.24±0.83)g/L,(299.3±341.5)cells/μL,(475.7±283.9)cells/μL,(142.8±218.6)cells/μL;ABO同型组患者则分别为(29.5±17.5)d,(31.1±40.5)U/L,(95.6±55.6)μmol/L,(11.8±3.0)g/L,(0.96±0.42)g/L,(397.3±250.9)cells/μL,(622.7±406.6)cells/μL,(190.7±216.6)cells/μL,以上指标两组间无统计学差异,t值分别为0.15,0.01,0.39,1.90,1.03,0.72,0.65,0.21,P均>0.05。③回顾性研究中有24人次的ABO次侧不相合血小板输注,未观察到急性溶血性输血反应发生。④模拟1治疗量的A型血小板输给B型(或AB型)成人后的红细胞凝集反应结果为阴性;模拟1治疗量的B型血小板输给A型(或AB型)成人后的红细胞凝集反应结果为阴性;模拟1治疗量的O型血小板输给A型(或B型或AB型)成人后的红细胞凝集反应结果为阴性。结论①ABO次侧不相合血小板与ABO同型血小板的临床输注疗效相当。②紧急特殊情况下输注不多于1治疗量ABO次侧不相合血小板未发现急性溶血性输血反应。